AI Article Synopsis

  • The scuticociliate Anophryoides haemophila is responsible for bumper car disease in American lobsters, and while its biology is somewhat understood, there’s limited molecular characterization available.
  • The research involved sequencing nearly 10,000 expressed sequence tags (ESTs) to analyze gene expression and discover new genes linked to its parasitic lifestyle, resulting in the identification of 843 clusters and unique sequences with some finding related to other ciliates like Tetrahymena.
  • The study found many genes related to cysteine proteases and suggested they could play a role in the disease, but gene expression analyses indicated no significant changes under different conditions, hinting at a potential opportunistic behavior of the parasite.

Article Abstract

The scuticociliate Anophryoides haemophila, causes bumper car disease in American lobster (Homarus americanus) in commercial holding facilities in Atlantic Canada. While the parasite has been recognized since the 1970s and much has been learned about its biology, minimal molecular characterization exists. With genome consortiums turning to model organisms like the ciliates Tetrahymena and Paramecium, the amount of relevant sequence data available has made sequence surveys more attractive for gene discovery in related ciliates. We sequenced 9984 expressed sequence tags (ESTs) from a non-normalized A. haemophila cDNA library to characterize gene expression patterns, functional gene distribution and to discover novel genes related to the parasitic life history. The A. haemophila ESTs were grouped into 843 clusters and singletons with 658 EST clusters having identifiable homologs, while 159 ESTs were unique and had no similarity to any sequences in the public databases. Not unexpectedly, about 67% of the A. haemophila ESTs have similarity to annotated and hypothetical genes from the related oligohymenophorean ciliate, Tetrahymena. Numerous cysteine proteases, hypothetical proteins and novel sequences possess putative secretory signal peptides suggesting that they may contribute to the pathogenesis of bumper car disease in lobster. Real time RT-qPCR analysis of cathepsin L and two homologs of cathepsin B did not show any changes in gene expression under varying in vitro growth conditions or during a modified-in vivo infection which may be suggestive of the opportunistic life history strategy of this ciliate.

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Source
http://dx.doi.org/10.1016/j.jip.2011.04.006DOI Listing

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